Sloviter R S
Neurology Research Center, Helen Hayes Hospital, New York State Department of Health, West Haverstraw 10993.
J Comp Neurol. 1989 Feb 8;280(2):183-96. doi: 10.1002/cne.902800203.
Two neuronal calcium-binding proteins, calbindin-D28k (CaBP) and parvalbumin (PV), were localized in the normal rat hippocampus by using immunocytochemical methods to determine 1) their location and 2) whether a correlation exists between the presence of these two calcium-binding proteins and the selective vulnerability of different hippocampal neuronal populations to experimental seizure activity. CaBP-like immunoreactivity (CaBP-LI) is present in all dentate granule cells and some, but not all, CA1 and CA2 pyramidal cells. Some CA1 pyramidal cells lack CaBP-LI, and those that do are lightly stained compared to the dentate granule cells. CA3 pyramidal cells appear to contain neither CaBP- nor PV-LI, and no granule or pyramidal cells exhibit PV-LI. CaBP-LI is present in distinct populations of dentate and hippocampal interneurons but absent from others. In area dentata, CaBP-LI is present in a small number of interneurons of the molecular and granule cell layers and in a small population of presumed basket cells in or below the granule cell layer. Conversely, more presumed dentate basket cells exhibit PV-LI than CaBP-LI. In the hilus of area dentata, few cells are CaBP- or PV-immunoreactive. The hilar somatostatin/neuropeptide Y (NPY)-immunoreactive cells and hilar mossy cells, two distinct and large populations, lack CaBP- and PV-LI. In the CA3 region, CaBP-LI is present in a relatively small number of interneurons in each stratum. PV-immunoreactive interneurons in area CA3 are more numerous. In area CA1, CaBP-LI is present in many interneurons in strata radiatum and lacunosum-moleculare. Some, but relatively fewer, CaBP-positive interneurons are present in strata pyramidale and oriens. Conversely, PV-immunoreactive interneurons are numerous in strata pyramidale and oriens but rare in strata radiatum and lacunosum-moleculare. Staining with the particulate chromagen benzidine hydrochloride revealed a previously undescribed dense band of CaBP-LI in the inner dentate molecular layer, a lamina enriched with kainate-displaceable glutamate-binding sites and innervated by the apparently excitatory ipsilateral associational/commissural (IAC) pathway that originates in the CaBP-negative hilar mossy cells. Bilateral electrical stimulation of the perforant path was performed in order to destroy the hilar mossy cells and to determine if this band of CaBP-LI is normally present within the mossy cell terminals. Perforant path stimulation that destroyed hilar mossy cells throughout the dorsal portions of both hippocampi did not abolish the dense CaBP-like immunoreactivity in the inner molecular layer.
采用免疫细胞化学方法,对正常大鼠海马中的两种神经元钙结合蛋白——钙结合蛋白-D28k(CaBP)和小白蛋白(PV)进行定位,以确定:1)它们的位置;2)这两种钙结合蛋白的存在与不同海马神经元群体对实验性癫痫活动的选择性易损性之间是否存在相关性。CaBP样免疫反应性(CaBP-LI)存在于所有齿状颗粒细胞以及部分(但并非全部)CA1和CA2锥体细胞中。一些CA1锥体细胞缺乏CaBP-LI,与齿状颗粒细胞相比,那些具有CaBP-LI的细胞染色较浅。CA3锥体细胞似乎既不含有CaBP-LI也不含有PV-LI,并且没有颗粒细胞或锥体细胞显示出PV-LI。CaBP-LI存在于齿状和海马中间神经元的不同群体中,而在其他群体中则不存在。在齿状回区域,CaBP-LI存在于分子层和颗粒细胞层的少数中间神经元以及颗粒细胞层或其下方的一小群假定的篮状细胞中。相反,显示PV-LI的假定齿状篮状细胞比显示CaBP-LI的更多。在齿状回的门区,很少有细胞具有CaBP或PV免疫反应性。门区生长抑素/神经肽Y(NPY)免疫反应性细胞和门区苔藓细胞这两个不同的大群体缺乏CaBP和PV-LI。在CA3区域,CaBP-LI存在于每个层中相对少数的中间神经元中。CA3区域中PV免疫反应性中间神经元更多。在CA1区域,CaBP-LI存在于辐射层和腔隙-分子层的许多中间神经元中。在锥体细胞层和原层中存在一些(但相对较少)CaBP阳性中间神经元。相反,PV免疫反应性中间神经元在锥体细胞层和原层中很多,但在辐射层和腔隙-分子层中很少见。用颗粒状显色剂盐酸联苯胺染色显示,在齿状回内分子层中有一条先前未描述的CaBP-LI致密带,该层富含可被 kainate 置换的谷氨酸结合位点,并由起源于CaBP阴性门区苔藓细胞的明显兴奋性同侧联合/连合(IAC)通路支配。为了破坏门区苔藓细胞并确定这条CaBP-LI带是否正常存在于苔藓细胞终末内,对穿通通路进行了双侧电刺激。破坏双侧海马背侧部分整个门区苔藓细胞的穿通通路刺激并没有消除内分子层中致密的CaBP样免疫反应性。
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